Downregulation of renal mrps transporters in acute lymphoblastic leukemia mediated by the il-6/stat3/pxr signaling pathway

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Abstract

Purpose: Considering prior investigations on reductions of renal multidrug resistance-associated protein (MRP) 2 and 4 transporters in mice with acute lymphoblastic leukemia (ALL), we sought to characterize the underlying mechanisms responsible for IL-6/STAT3/ PXR-mediated changes in the expression of MRP2 and MRP4 in ALL. Subjects and Methods: ALL xenograft models were established and intravenously injected with methotrexate (MTX) of MRPs substrate in NOD/SCID mice. Protein expression of MRPs and associated mechanisms were detected by Western blotting and immunocytochemistry. Plasma concentrations of MTX were determined using high-performance liquid chromatography-tandem mass spectrometry (HPLC-MS/MS). Results: Plasma IL-6 levels in patients with newly diagnosed ALL were increased compared to children with pneumonia. Similarly, plasma IL-6 levels in ALL, ALL-tocilizumab (TCZ, an IL-6 receptor inhibitor) and ALL-S3I-201 (a selective inhibitor of STAT3) mice were increased compared to the control group. The MRP2, MRP4, and PXR expression in HK-2 cells treated with IL-6 were decreased, whereas the p-STAT3 expression was significantly increased compared to the control group results. These results are consistent with clearance of MRPs-mediated MTX in the ALL group. These effects were attenuated by blocking IL-6/ STAT3/PXR signaling pathway. Conclusion: Inflammation-mediated changes in pharmacokinetics are thought to be executed through pathways IL-6-activated pathways, which can facilitate a better understanding of the potential for the use of IL-6 to predict the severity of adverse outcomes and the major implications on potential ALL treatments.

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Zhou, Y., Nie, A. Q., Chen, S., Wang, M. M., Yin, R., Tang, B. H., … Zhao, W. (2021). Downregulation of renal mrps transporters in acute lymphoblastic leukemia mediated by the il-6/stat3/pxr signaling pathway. Journal of Inflammation Research, 14, 2239–2252. https://doi.org/10.2147/JIR.S310687

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